Opin vísindi

Opin vísindi er varðveislusafn vísindaefnis og doktorsritgerða í opnum aðgangi á vegum íslenskra háskóla og Landsbókasafns Íslands - Háskólabókasafns.
Opinn aðgangur að rannsóknaniðurstöðum er í samræmi við 10. gr. laga nr. 3/2003 um opinberan stuðning við vísindarannsóknir sem og kröfur innlendra og erlendra rannsóknasjóða. Markmiðið með opnum aðgangi er að niðurstöður rannsókna séu aðgengilegar sem flestum óhindrað og án endurgjalds á rafrænu formi. Vistun í varðveislusafninu er varanleg og ætlað að tryggja aðgang að vísindaefni íslenskra háskóla í opnum aðgangi um ókomna tíð. Varðveislusafnið Opin vísindi er tengt við rannsóknagáttina IRIS og rannsóknaniðurstöður í opnum aðgangi sem eru skráðar í IRIS eru um leið vistaðar og gerðar aðgengilegar til framtíðar í varðveislusafninu. Með því að safna þessu efni saman í eitt safn verður aðgangur að því einfaldur og þægilegur fyrir alla sem vilja kynna sér það og geta þannig notið þess öfluga vísindastarfs sem fram fer í háskólum landsins.

Varðveislusafnið er OpenAIRE / OpenAIREplus samhæft og samrýmist kröfum sem gerðar eru um birtingu rannsóknaniðurstaðna úr verkefnum sem styrkt eru úr evrópsku rannsóknaáætlununum FP7 og H2020.

Varðveislusafnið notar opna hugbúnaðinn DSpace.

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Niðurstöður 1 - 9 af 9

Háskóli Íslands
University of Iceland
Háskólinn á Akureyri
University of Akureyri
Háskólinn á Bifröst
Bifröst University
Háskólinn á Hólum
Hólar University College
Háskólinn í Reykjavík
Reykjavík University
IRIS
IRIS
Landbúnaðarháskóli Íslands
Agricultural University of Iceland
Landsbókasafn Íslands - Háskólabókasafn
National and University Library of Iceland
Listaháskóli Íslands
Iceland University of the Arts

Nýlega bætt við

Verk

Melanoma risk and melanocyte biology

(2020) Bertrand, Juliette U.; Steingrimsson, Eirikur; Jouenne, Fanélie; Bressac-De Paillerets, Brigitte; Larue, Lionel; Faculty of Medicine

Cutaneous melanoma arises from melanocytes following genetic, epigenetic and allogenetic (i.e. other than epi/genetic) modifications. An estimated 10% of cutaneous melanoma cases are due to inherited variants or de novo mutations in approximately 20 genes, found using linkage, next-generation sequencing and association studies. Based on these studies, 3 classes of predisposing melanoma genes have been defined based on the frequency of the variants in the general population and lifetime risk of developing a melanoma: (i) ultra-rare variants with a high risk, (ii) rare with a moderate risk, and (iii) frequent variants with a low risk. Most of the proteins encoded by these genes have been shown to be involved in melanoma initiation, including proliferation and senescence bypass. This paper reviews the role(s) of these genes in the transformation of melanocytes into melanoma. It also describes their function in the establishment and renewal of melanocytes and the biology of pigment cells, if known.

Verk

BRN2 is a non-canonical melanoma tumor-suppressor

(2021-06-17) Hamm, Michael; Sohier, Pierre; Petit, Valérie; Raymond, Jérémy H.; Delmas, Véronique; Le Coz, Madeleine; Gesbert, Franck; Kenny, Colin; Aktary, Zackie; Pouteaux, Marie; Rambow, Florian; Sarasin, Alain; Charoenchon, Nisamanee; Bellacosa, Alfonso; Sanchez-del-Campo, Luis; Mosteo, Laura; Lauss, Martin; Meijer, Dies; Steingrímsson, Eiríkur; Jönsson, Göran B.; Cornell, Robert A.; Davidson, Irwin; Goding, Colin R.; Larue, Lionel; Faculty of Medicine

While the major drivers of melanoma initiation, including activation of NRAS/BRAF and loss of PTEN or CDKN2A, have been identified, the role of key transcription factors that impose altered transcriptional states in response to deregulated signaling is not well understood. The POU domain transcription factor BRN2 is a key regulator of melanoma invasion, yet its role in melanoma initiation remains unknown. Here, in a BrafV600EPtenF/+ context, we show that BRN2 haplo-insufficiency promotes melanoma initiation and metastasis. However, metastatic colonization is less efficient in the absence of Brn2. Mechanistically, BRN2 directly induces PTEN expression and in consequence represses PI3K signaling. Moreover, MITF, a BRN2 target, represses PTEN transcription. Collectively, our results suggest that on a PTEN heterozygous background somatic deletion of one BRN2 allele and temporal regulation of the other allele elicits melanoma initiation and progression.

Verk

Mental health challenges of young labor migrants from the healthcare professionals perspective : Lessons learned from a multi‐country meeting

(2021-09-21) Princeton, Daisy Michelle; Bregård, Ida Marie; Annion, Marianne; Shooghi, Gine; Rom, Gitte; Örlygsdóttir, Brynja; Sigurðardóttir, Hildur; Kuismin, Riita; Korhonen, Joonas; Kisa, Sezer; Faculty of Nursing and Midwifery

The mental health of young labor immigrants (YLI’s) is a public health issue that has become notably more apparent during the COVID‐19 pandemic. It is well established in the literature that most YLI’s are young and healthy when they arrive in the host country. However, due to the poor living and working conditions, as well as linguistic and socioeconomic barriers to health care in the host country, their physical and mental health often deteriorates. Between 1 March 2021 and 5 March 2021, a virtual meeting was organized by Oslo Metropolitan University in collaboration with the Nordic Council of Ministers mobility and network program for education in the Nordic and Baltic countries (Nordplus). It consisted of a multidisciplinary team of 26 participants from Nordic and Baltic countries. Topics included working and living conditions of YLI’s, prejudices towards immigrants, and mental health‐related interventions for YLI’s in the participating countries. This paper draws attention to some of the mental health challenges and needs of YLI’s and to the suggestions gathered from the Nordplus meeting to combat these challenges from a healthcare professional’s perspective.

Verk

Galectin 13 (PP13) facilitates remodeling and structural stabilization of maternal vessels during pregnancy

(2019-07-01) Sammar, Marei; Drobnjak, Tijana; Mandala, Maurizio; Gizurarson, Sveinbjörn; Huppertz, Berthold; Meiri, Hamutal; Faculty of Pharmaceutical Sciences; Health Sciences

Galectins regulate cell growth, proliferation, differentiation, apoptosis, signal transduction, mRNA splicing, and interactions with the extracellular matrix. Here we focus on the galectins in the reproductive system, particularly on a group of six galectins that first appears in anthropoid primates in conjunction with the evolution of highly invasive placentation and long gestation. Of these six, placental protein 13 (PP13, galectin 13) interacts with glycoproteins and glycolipids to enable successful pregnancy. PP13 is related to the development of a major obstetric syndrome, preeclampsia, a life-threatening complication of pregnancy which affects ten million pregnant women globally. Preeclampsia is characterized by hypertension, proteinuria, and organ failure, and is often accompanied by fetal loss and major newborn disabilities. PP13 facilitates the expansion of uterine arteries and veins during pregnancy in an endothelial cell-dependent manner, via the eNOS and prostaglandin signaling pathways. PP13 acts through its carbohydrate recognition domain that binds to sugar residues of extracellular and connective tissue molecules, thus inducing structural stabilization of vessel expansion. Further, decidual PP13 aggregates may serve as a decoy that induces white blood cell apoptosis, contributing to the mother’s immune tolerance to pregnancy. Lower first trimester PP13 level is one of the biomarkers to predict the subsequent risk to develop preeclampsia, while its molecular mutations/polymorphisms that are associated with reduced PP13 expression are accompanied by higher rates of preeclampsia We propose a targeted PP13 replenishing therapy to fight preeclampsia in carriers of these mutations.

Verk

Evaluation of in vitro mucoadhesiveness and texture profile analysis of doxycycline in situ hydrogels

(2020-01) Patlolla, V. G.R.; Holbrook, W. P.; Gizurarson, S.; Kristmundsdottir, P.; Faculty of Odontology; Faculty of Pharmaceutical Sciences

Delivery of active ingredients to the oral mucosa from topically applied formulations reduces side effects from systemic administration and enhances the treatment efficiency. The challenge however, is to maintain the formulation at the administration site due to rapid salivary flow and mechanical movements of the mouth. Therefore, addition of mucoadhesive polymers could aid in enhancing the formulation residence time by increasing the mucoadhesion capacity but this effect is negligible especially if low ratio of mucoadhesive polymers are added to the formulation. Different mucoadhesive polymers at 0.5% w/w (either single or combination of two polymers) were added to the hydrogels and tested for mucoadhesion capacity, tensile strengths, adhesiveness, cohesiveness, compressibility and hardness. 0.5% povidone showed significantly highest work of mucoadhesion, 0.5% Carbopol formulation showed least cohesiveness and 0.5% HPMC showed highest adhesiveness, but a formulation containing a combination of 0.25% HPMC and 0.25% povidone showed the ideal parameters among all the mucoadhesive polymers tested. The effect of increase in concentration of HPMC (0.5, 1, 1.5, 2%) showed linear relationship for work of mucoadhesion and tensile strengths whereas for TPA the values were non-linear. The drug release from the optimized polymer matrices was found to follow zero-order release profile and the mechanism was found to be super case-II transport relaxation release. The results of this study indicate the mucoadhesive polymers do not impact the tensile strengths (p=0.05), but the texture properties and work of mucoadhesion of the formulations can be significantly (p<0.05) altered by the choice of mucoadhesive component at 0.5%w/w, though not for all the polymers tested. The study provides scope to predict in vivo performance and helps optimize for localized delivery.